Enniatins A1, B and B1 from an endophytic strain of Fusarium tricinctum induce apoptotic cell death in H4IIE hepatoma cells accompanied by inhibition of ERK phosphorylation
Watjen, Wim and Debbab, Adbessamad and Hohlfeld, Anke and Chovolou, Yvonni and Kampkötter, Andreas and Edrada-Ebel, RuAngelie and Ebel, Rainer and Hakikj, Adbelhak and Mosaddak, Mahjouba and Totzke, Frank and Kubbutat, Michael H.G. and Proksch, Peter (2009) Enniatins A1, B and B1 from an endophytic strain of Fusarium tricinctum induce apoptotic cell death in H4IIE hepatoma cells accompanied by inhibition of ERK phosphorylation. Molecular Nutrition and Food Research, 53 (4). pp. 431-440. ISSN 1613-4125 (https://doi.org/10.1002/mnfr.200700428)
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Enniatins are mycotoxins which have important impact on human health, e.g. as contaminants of cereals, but also are discussed as possible anticancer agents. We investigated toxic effects of enniatins A1, B and B1 isolated from Fusarium tricinctum on different cancer cell lines. The enniatins showed moderate activity in HepG2 and C6 cells (EC50-values approximately 10-25 M), but were highly toxic in H4IIE cells (EC50-values approximately 1-2.5 M). In H4IIE cells, all enniatins increased caspase 3/7 activity and nuclear fragmentation as markers for apoptotic cell death. Enniatin A1, enniatin B1, and, to a lesser extent, also enniatin B decreased the activation of extracellular regulated protein kinase (ERK) (p44/p42), a mitogen-activated protein kinase which is associated with cell proliferation. Furthermore, enniatins A1 and B1, but not enniatin B were able to inhibit moderately tumor necrosis factor (TNF-)-induced NF-B activation. Screening of 24 additional protein kinases involved in signal transduction pathways (cell proliferation, survival, angiogenesis and metastasis) showed no inhibitory activity of enniatins. We conclude that enniatins A1 and B1 and, to a lesser extent, enniatin B may possess anticarcinogenic properties by induction of apoptosis and disruption of ERK signalling pathway. Further analysis of these substances is necessary to analyse their usefulness for cancer therapy.
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Item type: Article ID code: 13160 Dates: DateEventApril 2009Published8 December 2008Published OnlineSubjects: Medicine > Therapeutics. Pharmacology
Medicine > Pharmacy and materia medica
Science > MicrobiologyDepartment: Faculty of Science > Strathclyde Institute of Pharmacy and Biomedical Sciences Depositing user: Ms Ann Barker-Myles Date deposited: 06 Oct 2009 13:58 Last modified: 11 Nov 2024 09:08 URI: https://strathprints.strath.ac.uk/id/eprint/13160